VRP immunotherapy targeting neu: treatment efficacy and evidence for immunoediting in a stringent rat mammary tumor model

Laust, Amanda K.; Sur, Brandon W.; Wang, Kehui; Hubby, Bolyn; Smith, Jonathan; Nelson, Edward L.

doi:10.1007/s10549-007-9517-8

Cited by 13 publications

(13 citation statements)

References 74 publications

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“…It is important to note that these distal tissues were analyzed for the presence of VRP message and subsequently found to be completely devoid of replicon RNA, as measured by real-time PCR for VEE nsP1 message (data not shown). Lymph nodes other than the popliteal DLN are also consistently absent of viral antigen following VRP infection of mice, including the contralateral DLN (40,44).…”

Section: Resultsmentioning

confidence: 97%

“…Following footpad inoculation, Langerhans cells at the site of inoculation are the initial cells infected, rapidly migrating to the lymph node draining the injection site. As such, it is the DLN that serves as the earliest site for viral replication, not the tissue surrounding the inoculation site (40,44). Consequently, the earliest host response to VEE infection is established within the DLN, as demonstrated by the robust induction of the host antiviral gene response within the infected cells of the DLN (26,39).…”

Section: Resultsmentioning

confidence: 99%

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Acute Infection with Venezuelan Equine Encephalitis Virus Replicon Particles Catalyzes a Systemic Antiviral State and Protects from Lethal Virus Challenge

Konopka

Thompson

Whitmore

et al. 2009

J Virol

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The host innate immune response provides a critical first line of defense against invading pathogens, inducing an antiviral state to impede the spread of infection. While numerous studies have documented antiviral responses within actively infected tissues, few have described the earliest innate response induced systemically by infection. Here, utilizing Venezuelan equine encephalitis virus (VEE) replicon particles (VRP) to limit infection to the initially infected cells in vivo, a rapid activation of the antiviral response was demonstrated not only within the murine draining lymph node, where replication was confined, but also within distal tissues. In the liver and brain, expression of interferon-stimulated genes was detected by 1 to 3 h following VRP footpad inoculation, reaching peak expression of >100-fold over that in mock-infected animals. Moreover, mice receiving a VRP footpad inoculation 6, 12, or 24 h prior to an otherwise lethal VEE footpad challenge were completely protected from death, including a drastic reduction in challenge virus titers. VRP pretreatment also provided protection from intranasal VEE challenge and extended the average survival time following intracranial challenge. Signaling through the interferon receptor was necessary for antiviral gene induction and protection from VEE challenge. However, VRP pretreatment failed to protect mice from a heterologous, lethal challenge with vesicular stomatitis virus, yet conferred protection following challenge with influenza virus. Collectively, these results document a rapid modulation of the host innate response within hours of infection, capable of rapidly alerting the entire animal to pathogen invasion and leading to protection from viral disease.

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Section: Resultsmentioning

confidence: 97%

Section: Resultsmentioning

confidence: 99%

Acute Infection with Venezuelan Equine Encephalitis Virus Replicon Particles Catalyzes a Systemic Antiviral State and Protects from Lethal Virus Challenge

Konopka

Thompson

Whitmore

et al. 2009

J Virol

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“…During the experimental period, the tumor size was measured by a caliper. The breast cancer animal model was chosen since the model is a well-established animal model in breast cancer study (13762 MAT B-III breast cancer cell line is highly tumorigenic in Fischer 344 since the cell line is derived from the strain of Fischer 344 itself) [12][13][14]. Cyclophosphamide was used because the chemical has been used as a chemotherapeutic agent for treating human [15][16][17] and rat [14,18] breast tumors in previous researches.…”

Section: Animal Modelmentioning

confidence: 99%

Longitudinal Raman Spectroscopic Observation of Skin Biochemical Changes due to Chemotherapeutic Treatment for Breast Cancer in Small Animal Model

Seong

Myoung

Lee

et al. 2017

Journal of Spectroscopy

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The cancer field effect (CFE) has been highlighted as one of indirect indications for tissue variations that are insensitive to conventional diagnostic techniques. In this research, we had a hypothesis that chemotherapy for breast cancer would affect skin biochemical compositions that would be reflected by Raman spectral changes. We used a fiber-optic probe-based Raman spectroscopy to perform preliminary animal experiments to validate the hypothesis. Firstly, we verified the probing depth of the fiber-optic probe (~800 μm) using a simple intravenous fat emulsion-filled phantom having a silicon wafer at the bottom inside a cuvette. Then, we obtained Raman spectra during breast cancer treatment by chemotherapy from a small animal model in longitudinal manner. Our results showed that the treatment causes variations of biochemical compositions in the skin. For further validation, the Raman spectra will have to be collected from more populations and spectra will need to be compared with immunohistochemistry of the breast tissue.

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“…The high degree of homology with other receptor tyrosine kinases, including other members of the HER family, and the expression of HER2/neu in normal tissues, pose significant challenges that need to be addressed, including overcoming the anticipated immunological tolerance while maintaining specificity of the elicited immune response. Much of the preclinical work was performed in HER2/neu transgenic mouse models due, in part, to the fact that a murine homolog was not confirmed until the early 2000s [14][15][16], although other models were also employed (dog, guinea pig, rat, primate) [209][210][211][212][213][214]. The majority of these have focused on the extracellular domain of HER2/neu due, in large part to the high degree of homology of the intracellular kinase domain with other receptor tyrosine kinases both in and outside of the HER family [209,[215][216][217][218][219], although some strategies have included elements from the intracellular domain [213][214][215].…”

Section: Her2/neu Antigen-specific Immunotherapymentioning

confidence: 99%

“…Viral vector vaccine strategies using adenovirus vectors [257][258][259][260], alphavirus vectors [212,213,261], vaccinia virus vectors (NCT00485277 and NCT01152398), vesicular stomatitis virus [262] and polyoma virus systems [263,264] have all been used to elicit anti-HER2/neu immune responses. The intracellular bacteria Listeria monocytogenes has also been adapted as an immunotherapeutic vector system and studied in strategies to elicit anti-HER2/neu immune responses [215,265].…”

Section: Her2/neu Antigen-specific Immunotherapymentioning

confidence: 99%

HER2/neu: an increasingly important therapeutic target. Part 1: basic biology & therapeutic armamentarium

Nelson¹

2014

Clinical Investigation

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VRP immunotherapy targeting neu: treatment efficacy and evidence for immunoediting in a stringent rat mammary tumor model

Cited by 13 publications

References 74 publications

Acute Infection with Venezuelan Equine Encephalitis Virus Replicon Particles Catalyzes a Systemic Antiviral State and Protects from Lethal Virus Challenge

Acute Infection with Venezuelan Equine Encephalitis Virus Replicon Particles Catalyzes a Systemic Antiviral State and Protects from Lethal Virus Challenge

Longitudinal Raman Spectroscopic Observation of Skin Biochemical Changes due to Chemotherapeutic Treatment for Breast Cancer in Small Animal Model

HER2/neu: an increasingly important therapeutic target. Part 1: basic biology & therapeutic armamentarium

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